Identifying The Genes Responsible For Autism Disorders Is Critical For Diagnosis And Treatment
Main Category: AutismArticle Date: 04 Feb 2013 - 2:00 PST
Identifying The Genes Responsible For Autism Disorders Is Critical For Diagnosis And Treatment
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Autism spectrum disorders affect nearly 1 in 88 children, with symptoms ranging from mild personality traits to severe intellectual disability and seizures. Understanding the altered genetic pathways is critical for diagnosis and treatment. New work to examine which genes are responsible for autism disorders were presented at the 57th Annual Meeting of the Biophysical Society (BPS), held Feb. 2-6, 2013, in Philadelphia, Pa.
"Autism is the most inheritable of neurodevelopmental disorders," explains Rajini Rao of Johns Hopkins University in Baltimore, Md., "but identifying the underlying genes is difficult since no single gene contributes more than a tiny fraction of autism cases." Rather, she continues, "mutations in many different genes variably affect a few common pathways."
A team of scientists at Johns Hopkins and Tel Aviv University in Israel looked at genetic variations in DNA sequence in the ion transporter NHE9 and found that autism-associated variants in NHE9 result in a profound loss of transporter function. "Altering levels of this transporter at the synapse may modulate critical proteins on the cell surface that bring in nutrients or neurotransmitters such as glutamate," says Rao. "Elevated glutamate levels are known to trigger seizures, possibly explaining why autistic patients with mutations in these ion transporters also have seizures."
A unique aspect of the team's approach was that they exploited decades of basic research done in bacteria and yeast to study a complex human neurological disorder. First, the group at Tel Aviv University, led by Nir Ben-Tal, built structural models of NHE9 using a bacterial relative as a template, allowing the Rao laboratory at Johns Hopkins to use the simple baker's yeast for screening the mutations. In the future, as genomic information becomes readily available for everyone, such easy, inexpensive, and rapid screening methods will be essential to evaluate rare genetic variants in autism and other disorders.
Rao and her team are optimistic about the potential benefits of their latest findings. "Although the research is still at an early stage, drugs that target the cellular pathways regulated by NHE9 could compensate for its loss of function and lead to potential therapy in the future," Rao says. "These findings add a new candidate for genetic screening of at-risk patients that may lead to better diagnosis or treatment of autism."
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This news release was prepared for the Biophysical Society (BPS) by the American Institute of Physics (AIP).
The 57th Annual Meeting will be held at the Pennsylvania Convention Center (1101 Arch Street, Philadelphia, PA 19107). For maps and directions, please visit: http://www.paconvention.com/explore- philadelphia/directions-and-parkingg.
QUICK LINKS
Meeting Home Page: http://www.biophysics.org/2013meeting/Main/tabid/35 23/Default.aspx
Housing and Travel Information: http://www.biophysics.org/2013meeting/Accommodation sTravel/HotelInformation/tabid/3621/Default.aspx
Program Abstracts and Itinerary Planner: http://www.abstractsonline.com/plan/start.aspx? mkey=%7B763246BB-EBE4-430F-9545-81BC84D0C68C%7D
American Institute of Physics
MLA
23 May. 2013. <http://www.medicalnewstoday.com/releases/255810.php>
APA
http://www.medicalnewstoday.com/releases/255810.php.
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Visitor Opinions (latest shown first)
Weak study
posted by Payman on 5 Feb 2013 at 9:26 pmI am sorry to say but the study and researchers seem very wrong. They say "Autism is the most inheritable of neurodevelopmental disorders" but every one knows that genetic basis applies only to 15% of all autism cases. How do you make an statement like that when you do have no numbers to back it up.
In addition, this study does not relate to any specific subcategories of autism (Aspergers, regressive autism, PDD etc) since it seems as if there are various paths to autism. You cannot just pool them since they dont have the same medical pathology. Therefore their research means nothing no matter whatever transporter they might have found.
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